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Trial Outcomes & Findings for A Study To Evaluate The Safety And Efficacy Of PF-04958242 In Subjects With Cognitive Impairment Associated With Schizophrenia (CIAS) (NCT NCT02855411)

NCT ID: NCT02855411

Last Updated: 2020-01-09

Results Overview

The MCCB is a cognitive battery to assess 7 domains recommended by the MATRICS initiative (ie, working memory, verbal learning, speed of processing, attention/vigilance, visual learning, social cognition, reasoning and problem solving). The MCCB yields scores for individual tests that assess specific cognitive domains as well as a composite score. Scores for the individual tests and the overall composite score for all tests are calculated according to the developers' recommended scoring algorithms.

Recruitment status

TERMINATED

Study phase

PHASE2

Target enrollment

35 participants

Primary outcome timeframe

Baseline, Week 2, Week 6, Week 12

Results posted on

2020-01-09

Participant Flow

A total of 35 participants were screened before study termination.

No participants had been randomized to receive study drug or placebo before study termination.

Participant milestones

Participant milestones
Measure
Overall (PF-04958242/Placebo)
Participants were to take PF-04958242 0.15 milligram (mg), or PF-04958242 0.5 mg, or the matched placebo twice daily (BID) for approximately 85 consecutive days, with the last dose taken in the morning on Day 85.
Overall Study
STARTED
35
Overall Study
Assigned to Study Treatment
0
Overall Study
COMPLETED
0
Overall Study
NOT COMPLETED
35

Reasons for withdrawal

Reasons for withdrawal
Measure
Overall (PF-04958242/Placebo)
Participants were to take PF-04958242 0.15 milligram (mg), or PF-04958242 0.5 mg, or the matched placebo twice daily (BID) for approximately 85 consecutive days, with the last dose taken in the morning on Day 85.
Overall Study
Study terminated by sponsor
21
Overall Study
Does not meet entrance criteria
14

Baseline Characteristics

A Study To Evaluate The Safety And Efficacy Of PF-04958242 In Subjects With Cognitive Impairment Associated With Schizophrenia (CIAS)

Baseline characteristics by cohort

Baseline characteristics by cohort
Measure
Overall (PF-04958242/Placebo)
n=35 Participants
Participants were to take PF-04958242 0.15 milligram (mg), or PF-04958242 0.5 mg, or the matched placebo twice daily (BID) for approximately 85 consecutive days, with the last dose taken in the morning on Day 85.
Age, Continuous
41.4 years
STANDARD_DEVIATION 6.8 • n=113 Participants
Sex: Female, Male
Female
13 Participants
n=113 Participants
Sex: Female, Male
Male
22 Participants
n=113 Participants

PRIMARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The MCCB is a cognitive battery to assess 7 domains recommended by the MATRICS initiative (ie, working memory, verbal learning, speed of processing, attention/vigilance, visual learning, social cognition, reasoning and problem solving). The MCCB yields scores for individual tests that assess specific cognitive domains as well as a composite score. Scores for the individual tests and the overall composite score for all tests are calculated according to the developers' recommended scoring algorithms.

Outcome measures

Outcome data not reported

PRIMARY outcome

Timeframe: Baseline, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The UPSA-VIM is a functional capacity measure of 5 general skills that were previously identified as essential to functioning in the community: general organization, finance, social/communications, transportation, and household chores. The UCSD Performance Based Skills Assessment involves role play tasks that are administered as simulations of events that the person might encounter in the community.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

SARA is a clinical scale that is based on a semi--quantitative assessment of cerebellar ataxia on an impairment level and complements the brief neurological examination. The SARA has 8 items that are related to gait, stance, sitting, speech, finger-chase test, nose-finger test, fast alternating movements and heel-shin test.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, followed by weekly (Weeks 1 throughout 12), and 28 days after last dose

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

C-SSRS responses are mapped to the Columbia Classification Algorithm of Suicide Assessment (C-CASA). C-SSRS assesses whether participant experienced following: completed suicide (Category 1); suicide attempt (Category 2) (response of "Yes" on "actual attempt"); preparatory acts toward imminent suicidal behavior (Category 3) ("Yes" on "aborted attempt", or "interrupted attempt", or "preparatory acts or behavior"); suicidal ideation (Category 4) ("Yes" on "wish to be dead", or "non-specific active suicidal thoughts", or "active suicidal ideation with methods without intent to act or some intent to act, without specific plan or with specific plan and intent"); self-injurious behavior, no suicidal intent (Category 7) ("Yes" on "has participant engaged in non-suicidal self-injurious behavior"). Number of participants with "Yes" response for above mentioned categories was to be assessed.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The MCCB is a cognitive battery to assess 7 domains recommended by the MATRICS initiative (ie, working memory, verbal learning, speed of processing, attention/vigilance, visual learning, social cognition, reasoning and problem solving). The MCCB yields scores for individual tests that assess specific cognitive domains as well as a composite score. Scores for the individual tests and the overall composite score for all tests are calculated according to the developers' recommended scoring algorithms. The MCCB neurocognitive score contains all of the tests and domains of the MCCB composite score with the exception of social cognition.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The MCCB is a cognitive battery to assess 7 domains recommended by the MATRICS initiative (ie, working memory, verbal learning, speed of processing, attention/vigilance, visual learning, social cognition, reasoning and problem solving). The MCCB yields scores for individual tests that assess specific cognitive domains as well as a composite score. Scores for the individual tests and the overall composite score for all tests are calculated according to the developers' recommended scoring algorithms.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The MCCB is a cognitive battery to assess 7 domains recommended by the MATRICS initiative (ie, working memory, verbal learning, speed of processing, attention/vigilance, visual learning, social cognition, reasoning and problem solving). The MCCB yields scores for individual tests that assess specific cognitive domains as well as a composite score. Scores for the individual tests and the overall composite score for all tests are calculated according to the developers' recommended scoring algorithms.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The SCI-PANSS includes 3 scales and 30 items: 7 items that make up the Positive Scale; 7 items that make up the Negative Scale; and 16 items that make up the General Psychopathology Scale. The sum of the 30 items is defined as the total score.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The SCI--PANSS includes 3 scales and 30 items: 7 items that make up the Positive Scale; 7 items that make up the Negative Scale; and 16 items that make up the General Psychopathology Scale. The Subscale scores are the sum of corresponding individual items.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Baseline, Week 2, Week 6, Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The CGI--S consists of a single 7 point rating score of illness severity. Raters select 1 response based on the following question, "Considering your total clinical experience with this particular population, how mentally ill is your patient at this time?" Scores are: 1=Normal, not ill at all; 2=Borderline mentally ill; 3=Mildly ill; 4=Moderately ill; 5=Markedly ill; 6=Severely ill; or 7=Among the most severely ill participants.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Week 12

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The CGI-I consists of a single 7 point rating score total improvement, regardless of whether or not the change is due entirely to drug treatment. Raters select 1 response based on the following question, "Compared to your patient's condition at the beginning of treatment, how much has your patient changed?" Scores are: 1=Very much improved; 2=Much improved; 3=Minimally improved; 4=No change; 5=Minimally worse; 6=Much worse; or 7=Very much worse. For the CGI-I, the participant's condition at the Day 1 (baseline) visit is the criterion for judging improvement at subsequent visits.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: For AEs, the time frame was from taking first dose through and including last visit (28 days after the last dose), up to 113 days. For SAEs, the time frame was from the time that the participant provided informed consent to last visit, up to 143 days.

Population: Study was terminated before participants were treated. No AE data was collected and there were no SAEs reported during the screening phase.

An AE was any untoward medical occurrence in a participant who received study treatment without regard to possibility of causal relationship. AEs comprised both SAEs and non-SAEs. An SAE was an AE resulting in any of the following outcomes or deemed significant for any other reason: death; initial or prolonged inpatient hospitalization; life-threatening experience (immediate risk of dying); persistent or significant disability/incapacity; congenital anomaly. All AEs (serious and non-serious) occurring following start of treatment or increasing in severity in any period were to be considered as a treatment emergent AE.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Screening up to Week 12 or early termination

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

Number of participants with laboratory test abnormalities without regard to baseline abnormality is assessed. Laboratory test parameters include hematology, clinical chemistry, urinalysis, follicle stimulating hormone, urine drug screen, and pregnancy test.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Screening up to Week 12 or early termination

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

ECG criteria of potential clinical concern: 1) QRS interval (time from ECG Q wave to the end of the S wave corresponding to ventricle depolarization): greater than or equal to (\>=) 140 milliseconds (msec), \>=50% increase from baseline; 2) PR interval (the interval between the start of the P wave and the start of the QRS complex, corresponding to the time between the onset of the atrial depolarization and onset of ventricular depolarization): \>=300 msec, \>=25% increase when baseline is greater than (\>) 200 msec or \>=50% increase when baseline is less than or equal to (\<=) 200 msec; 3) QTcF interval (time from ECG Q wave to the end of the T wave corresponding to electrical systole corrected using Fridericia's formula): absolute value of 450 to less than (\<) 480 msec, 480 to \<500 msec, \>=500 msec; an increase from baseline of 30 to \<60 msec or \>=60 msec.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Screening up to Week 12 or early termination

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

Vital signs criteria of potential clinical concern: 1) systolic blood pressure \<90 millimeters of mercury (mm Hg); 2) change from baseline of systolic blood pressure \>=30 mm Hg; 3) diastolic blood pressure \<50 mm Hg; 4) change from baseline of diastolic blood pressure \>=20 mm Hg; 5) supine pulse rate \<40 or \>120 beats per minute (bpm); 6) standing pulse rate \<40 or \>140 bpm.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Screening up to Week 12 or early termination

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

The extended neurological examination includes observation for cerebellar (intention) tremor and for non-cerebellar tremors (eg, resting or positional), finger nose, heel shin, Romberg, tandem walking, positional and gaze-evoked nystagmus, reflexes, muscle strength, cranial nerves, sensory function of upper and lower extremities. The brief neurological examination includes an assessment of motor and sensory function, cranial nerves, reflexes, non-cerebellar tremor (eg, resting or positional) and cerebellar function. The assessment of cerebellar function is complemented by the Scale for the Assessment and Rating of Ataxia (SARA), a clinical scale based on a semi-quantitative assessment of cerebellar ataxia on an impairment level.

Outcome measures

Outcome data not reported

SECONDARY outcome

Timeframe: Screening up to Week 12 or early termination

Population: Study was terminated before participants were treated and no data was collected for the endpoints.

A full physical examination includes head, ears, eyes, nose, mouth, skin, heart and lung examinations, lymph nodes, gastrointestinal, musculoskeletal, and neurological systems. The brief physical examination is focused on general appearance, the respiratory and cardiovascular systems, as well as towards participant reported symptoms.

Outcome measures

Outcome data not reported

Adverse Events

Overall (PF-04958242/Placebo)

Serious events: 0 serious events
Other events: 0 other events
Deaths: 0 deaths

Serious adverse events

Adverse event data not reported

Other adverse events

Adverse event data not reported

Additional Information

Biogen Study Medical Director

Biogen

Phone: 866-633-4636

Results disclosure agreements

  • Principal investigator is a sponsor employee Pfizer has the right to review disclosures, requesting a delay of less than 60 days. Investigator will postpone single center publications until after disclosure of pooled data (all sites), less than 12 months from study completion/termination at all participating sites. Investigator may not disclose previously undisclosed confidential information other than study results.
  • Publication restrictions are in place

Restriction type: OTHER